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Immune synapse formation promotes lipid peroxidation and MHC-I upregulation in licensed dendritic ce...

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Immune synapse formation promotes lipid peroxidation and MHC-I upregulation in licensed dendritic ce...

https://devfeature-collection.sl.nsw.gov.au/record/TN_cdi_doaj_primary_oai_doaj_org_article_575e9711ad8c4a6bab6822f8ba691d6a

Immune synapse formation promotes lipid peroxidation and MHC-I upregulation in licensed dendritic cells for efficient priming of CD8+ T cells

About this item

Full title

Immune synapse formation promotes lipid peroxidation and MHC-I upregulation in licensed dendritic cells for efficient priming of CD8+ T cells

Author / Creator

Calzada-Fraile, Diego , Iborra, Salvador , Ramírez-Huesca, Marta , Jorge, Inmaculada , Dotta, Enrico , Hernández-García, Elena , Martín-Cófreces, Noa , Nistal-Villán, Estanislao , Veiga, Esteban , Vázquez, Jesús , Pasqual, Giulia and Sánchez-Madrid, Francisco

Publisher

London: Nature Publishing Group UK

Journal title

Nature communications, 2023-10, Vol.14 (1), p.6772-6772, Article 6772

Language

English

Formats

Articles

Publication information

Publisher

London: Nature Publishing Group UK

Subjects

More information

Scope and Contents

Contents

Antigen cognate dendritic cell (DC)-T cell synaptic interactions drive activation of T cells and instruct DCs. Upon receiving CD4
+
T cell help, post-synaptic DCs (psDCs) are licensed to generate CD8
+
T cell responses. However, the cellular and molecular mechanisms that enable psDCs licensing remain unclear. Here, we describe that anti...

Alternative Titles

Full title

Immune synapse formation promotes lipid peroxidation and MHC-I upregulation in licensed dendritic cells for efficient priming of CD8+ T cells

Authors, Artists and Contributors

Author / Creator

Identifiers

Primary Identifiers

Record Identifier

TN_cdi_doaj_primary_oai_doaj_org_article_575e9711ad8c4a6bab6822f8ba691d6a

Permalink

https://devfeature-collection.sl.nsw.gov.au/record/TN_cdi_doaj_primary_oai_doaj_org_article_575e9711ad8c4a6bab6822f8ba691d6a

Other Identifiers

ISSN

2041-1723

E-ISSN

2041-1723

DOI

10.1038/s41467-023-42480-3

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